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Med12 is essential for early mouse development and for canonical Wnt and Wnt/PCP signaling.

机译:med12对早期发育和经典Wnt和Wnt / pCp信号传导至关重要。

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摘要

The Mediator complex is commonly seen as a molecular bridge that connects DNA-bound transcription factors to the RNA polymerase II (Pol II) machinery. It is a large complex of 30 subunits that is present in all eukaryotes. The Med12 subunit has been implicated not only in the regulation of Pol II activity, but also in the binding of transcription factors to the bulk of the Mediator complex. We targeted Med12 in mouse embryonic stem cells to investigate the in vivo function of this subunit. We report here the developmental defects of Med12 hypomorphic mutants that have a drastic reduction in Med12 protein levels. These mutants fail to develop beyond embryonic day 10 and have severe defects in neural tube closure, axis elongation, somitogenesis and heart formation. We show that in Med12 hypomorphic embryos, the Wnt/planar cell polarity pathway is disrupted and that canonical Wnt/β-catenin signaling is impaired. In agreement with this, embryos that are incapable of Med12 expression failed to establish the anterior visceral endoderm or activate brachyury expression, and did not complete gastrulation.
机译:介体复合物通常被视为将DNA结合的转录因子连接到RNA聚合酶II(Pol II)机制的分子桥。它是所有真核生物中都存在的由30个亚基组成的大型复合体。 Med12亚基不仅与Pol II活性的调节有关,而且与转录因子与大部分介体复合物的结合有关。我们将Med12靶向小鼠胚胎干细胞,以研究该亚基的体内功能。我们在这里报告Med12蛋白亚型突变的发展缺陷,该缺陷已大大降低了Med12蛋白水平。这些突变体不能在胚胎第10天后发育,并且在神经管闭合,轴伸长,体细胞发生和心脏形成方面存在严重缺陷。我们显示,在Med12亚型胚胎中,Wnt /平面细胞极性途径受到破坏,并且经典Wnt /β-catenin信号传导受到损害。与此相符的是,不能进行Med12表达的胚胎无法建立前内脏内胚层或激活腕膜上的表达,并且不能完全形成胃。

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